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钙拮抗剂对充血性心力衰竭的疗效

Usefulness of calcium antagonists for congestive heart failure.

作者信息

Colucci W S

出版信息

Am J Cardiol. 1987 Jan 30;59(3):52B-58B. doi: 10.1016/0002-9149(87)90082-8.

Abstract

In patients with congestive heart failure (CHF) due to dilated cardiomyopathy, nifedipine, diltiazem and several of the newer calcium antagonists including nicardipine, nitrendipine, felodipine and PN 200-110 (isradipine) improve left ventricular function. Because of its relatively more pronounced negative inotropic and chronotropic actions, verapamil is generally not tolerated by patients with left ventricular failure. In addition, even relatively vascular-selective agents such as nifedipine can occasionally cause significant left ventricular depression, particularly if combined with beta-adrenergic blocking agents. Comparative studies using nitroprusside to cause an equivalent decrease in arterial pressure indicate that nifedipine acts predominantly on the arterial vasculature, and that a small but significant decrease in contractility occurs, apparently due to a direct myocardial action. Although diltiazem causes a depression in myocardial contractility in dogs with volume overload heart failure, limited data show no significant negative inotropic action in patients with heart failure. The negative inotropic effects, if any, of newer and possibly more vascular-selective agents are not yet known. Calcium antagonists appear to act predominantly on the limb and coronary vasculature, with relatively less effect on renal and hepatic vessels. In patients with CHF, nifedipine causes an increase in coronary blood flow and a decrease in the aorto-coronary sinus oxygen difference indicating an improvement in myocardial energetics. Although nifedipine causes an increase in cardiac index and decreases in systemic vascular resistance and pulmonary capillary wedge pressure during exercise, the limited data available fail to show a short- or long-term increase in exercise capacity. Nifedipine causes an increase in plasma renin activity, possibly due to a direct action on the kidney.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在因扩张型心肌病导致的充血性心力衰竭(CHF)患者中,硝苯地平、地尔硫䓬以及包括尼卡地平、尼群地平、非洛地平和PN 200 - 110(伊拉地平)在内的几种新型钙拮抗剂可改善左心室功能。由于维拉帕米具有相对更明显的负性肌力和负性变时作用,左心室衰竭患者通常不耐受。此外,即使是相对具有血管选择性的药物如硝苯地平,偶尔也会导致显著的左心室功能抑制,尤其是与β - 肾上腺素能阻滞剂合用时。使用硝普钠使动脉压等效降低的对比研究表明,硝苯地平主要作用于动脉血管系统,并且出现了轻微但显著的收缩力下降,这显然是由于直接的心肌作用。尽管地尔硫䓬会使容量超负荷心力衰竭犬的心肌收缩力降低,但有限的数据表明,在心力衰竭患者中它没有显著的负性肌力作用。新型且可能更具血管选择性的药物的负性肌力作用(若有)尚不清楚。钙拮抗剂似乎主要作用于肢体和冠状动脉血管,对肾血管和肝血管的作用相对较小。在CHF患者中,硝苯地平可使冠状动脉血流量增加,主动脉 - 冠状窦氧分压差降低,这表明心肌能量代谢得到改善。尽管硝苯地平在运动期间会使心脏指数增加,全身血管阻力和肺毛细血管楔压降低,但现有的有限数据未能显示运动能力有短期或长期的提高。硝苯地平可使血浆肾素活性增加,这可能是由于对肾脏的直接作用。(摘要截选至250字)

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